✦ LIBER ✦

Characterization of the nuclear matrix proteins in a transgenic mouse model for prostate cancer

✍ Scribed by Eddy S. Leman; Julie A. Arlotti; Rajiv Dhir; Norman Greenberg; Robert H. Getzenberg

Publisher: John Wiley and Sons
Year: 2002
Tongue: English
Weight: 637 KB
Volume: 86
Category: Article
ISSN: 0730-2312
DOI: 10.1002/jcb.10216

No coin nor oath required. For personal study only.

✦ Synopsis

The nuclear matrix (NM) contains a number of proteins that have been found to be associated with transformation. We have previously identified changes in the NM associated with prostate cancer. In this study, we examine the molecular changes that are associated with prostate cancer development in transgenic adenocarcinoma of mouse prostate (TRAMP) model by studying the differences in the NM proteins (NMPs). We collected prostates from the TRAMP males at six critical time points: 6 weeks (puberty), 11 and 19 weeks (development of mild hyperplasia), 25 weeks (development of severe hyperplasia), 31 and 37 weeks (development of neoplasia). The nuclear matrices from the prostates collected at these time points were then isolated and the NMPs were characterized by high-resolution two-dimensional gel electrophoresis. We found three NMPs (E1A, E1B, and E1C) that were present in the 6-week-old prostate and two NMPs (E2A and E2B) that were present in the 11-week-old prostate. These NMPs were absent in the 31- and 37-week-old prostate. We also found five NMPs (E3A-E3E) that were present in the 31-week-old prostate, but absent in the earlier time points. In addition, three NMPs (Le1, Le2, Le3) were present at higher expression in the 6-, 11-, 19-, and 25-weeks old TRAMP prostates, but they were expressed lower during the development of neoplasia at 31- and 37-weeks old. Identification of these NMPs permits the development of novel markers that can characterize various stages of prostate cancer development as well as potentially therapeutic targets.

📜 SIMILAR VOLUMES

Nuclear matrix localization of high mobi

Nuclear matrix localization of high mobility group protein I(Y) in a transgenic mouse model for prostate cancer

✍ Eddy S. Leman; Michael C. Madigan; Gisela Brünagel; Natsuki Takaha; Donald S. Co 📂 Article 📅 2002 🏛 John Wiley and Sons 🌐 English ⚖ 332 KB

## Abstract Nuclear shape and the underlying nuclear structure, the nuclear matrix in cancer cells. Since the NM composition is considered to maintain nuclear shape and architecture, nuclear matrix proteins (NMPs) may be involved in transformation. Our laboratory has recently characterized a subset

Changes in the expression of cytokeratin

Changes in the expression of cytokeratins and nuclear matrix proteins are correlated with the level of differentiation in human prostate cancer

✍ Ingles Alberti; Paola Barboro; Marta Barbesino; Paola Sanna; Livia Pisciotta; Si 📂 Article 📅 2000 🏛 John Wiley and Sons 🌐 English ⚖ 574 KB

Generation and characterization of brain

Generation and characterization of brain lipid-binding protein promoter-based transgenic mouse models for the study of radial glia

✍ Ralf S. Schmid; Yukako Yokota; E. S. Anton 📂 Article 📅 2006 🏛 John Wiley and Sons 🌐 English ⚖ 827 KB

## Abstract Radial glia play an essential role in the generation of the cerebral cortex through their function as neuronal precursors and as neuronal migration guides. A molecular marker for radial glia in the developing central nervous system is the brain lipid‐binding protein (BLBP). To generate

Expression of the human cachexia-associa

Expression of the human cachexia-associated protein (HCAP) in prostate cancer and in a prostate cancer animal model of cachexia

✍ Zejing Wang; Eva Corey; G. Michael Hass; Celestia S. Higano; Lawrence D. True; D 📂 Article 📅 2003 🏛 John Wiley and Sons 🌐 French ⚖ 1014 KB

## Abstract Prostate cancer (CaP) patients with disseminated disease often suffer from severe cachexia, which contributes to mortality in advanced cancer. Human cachexia‐associated protein (HCAP) was recently identified from a breast cancer library based on the available 20‐amino acid sequence of p

Gene-directed enzyme prodrug therapy for

Gene-directed enzyme prodrug therapy for prostate cancer in a mouse model that imitates the development of human disease

✍ Rosetta Martiniello-Wilks; Allison Dane; Dale J. Voeks; Geetha Jeyakumar; Elin M 📂 Article 📅 2004 🏛 John Wiley and Sons 🌐 English ⚖ 310 KB 👁 1 views

## Abstract ## Background Gene‐directed enzyme prodrug therapy (GDEPT) based on the __E. coli__ enzyme purine nucleoside phosphorylase (PNP) represents a new approach for treating slow growing tumours like prostate cancer (PCa). Expressed enzyme converts a systemically administered prodrug, fludar

Synthetic matrix metalloproteinase inhib

Synthetic matrix metalloproteinase inhibitor, BB-94, inhibits the invasion of neoplastic human prostate cells in a mouse model

✍ Knox, J. David; Bretton, Louis; Lynch, Tamara; Bowden, G. Tim; Nagle, Ray B. 📂 Article 📅 1998 🏛 John Wiley and Sons 🌐 English ⚖ 214 KB 👁 1 views

## Background: It has been suggested that increased metalloproteinase activity is a critical event in neoplastic progression leading to the initiation of local invasion and ultimately to the dissemination of neoplastic cells. this has led to an interest in testing the ability of metalloproteinase i